Pulse oximetry

1. Pulse oximetry provides continuous measurement of a patient’s oxygenation status.

2. Measurements are obtained via sensors placed on the patient’s fingertip, earlobe, or forehead. These sensors use two light-emitting electrodes.

   1. The first emits red light that has a wavelength of 660 nm.

   2. The second emits infrared light that has a wavelength of 905, 910, or 940 nm.

   3. The difference in absorption of the red light and infrared light determines the oxyhemoglobin to deoxyhemoglobin ratio. This measurement corresponds to the pulse oximeter saturation estimate (SpO₂).

3. Pitfalls:

   1. Once the arterial oxygen saturation (SaO₂) falls below 70%, the pulse oximetry readings are no longer accurate.

   2. Pulse oximetry cannot reliably detect hypoxemia in the setting of carbon monoxide poisoning because carboxyhemoglobin has similar light absorption to that of oxyhemoglobin at 660 nm.

   3. It is also inaccurate in the setting of methemoglobinemia as both red light and infrared light are equally absorbed by methemoglobin. This results in a fixed SpO₂ around 85% regardless of the true SaO₂.

   4. Oxygenated blood that is redistributed from central to peripheral circulation can cause a delay in saturation readings known as pulse oximetry lag. This lag can be as long as 2–3 minutes in critically ill patients secondary to reduced blood flow.

   5. A proper waveform must be visualized on the monitor in order to be able to properly determine the SpO₂.

   6. Hypothermia and peripheral vasoconstriction can lead to inaccurate or unobtainable values.

End-tidal carbon dioxide (EtCO₂)

1. Capnography measures the partial pressure or concentration of expired carbon dioxide (CO₂), the EtCO₂. This concentration is a function of the production of CO₂ at the tissue level and delivery of CO₂ to the lungs by the circulatory system. Therefore, capnography provides important information regarding ventilation, circulation, and metabolism.

2. The normal expired CO₂ level is around 5%, which is approximately 40 mmHg.

3. There are two different EtCO₂ monitoring modalities that are used in the emergency department (ED).

   1. Colorimetric capnometry is a filter generally used to confirm endotracheal tube (ET) placement in the trachea.

      1. The filter attaches to the ET tube and displays the change in concentration of carbon dioxide by color change.

      2. In certain colorimetric capnometers, detection of carbon dioxide is exhibited by filter color change from purple to yellow. This is a semiquantitative mode of monitoring. The color ranges are as follows: purple = EtCO₂ <0.5%; tan = EtCO₂ 0.5–2%; and yellow = EtCO₂ >2%.

      3. Pitfalls:

         1. The filter can turn yellow when exposed to acidic material such as stomach contents, or medications including lidocaine and epinephrine.

         2. In patients in cardiac arrest, color change may not be seen even with tracheal intubation because of the low EtCO₂ value resulting from poor or absent blood flow.

   2. Quantitative capnography uses infrared technology to provide a continuous numerical value and a continuous waveform display of EtCO₂. This measure is plotted graphically on a monitor.

4. Some ED applications of quantitative EtCO₂ monitoring are listed below.

   1. Intubation:

      1. Quantitative EtCO₂ will reliably confirm tracheal placement of endotracheal tube despite low cardiac output states, unlike colorimetric devices.

      2. Postintubation continuous capnography can help early identification of airway obstruction or tube dislodgment.

   2. Procedural sedation:

      1. Pulse oximetry provides information about oxygenation, not ventilation. With any amount of supplemental oxygenation, detection of hypoventilation will be significantly delayed. This occurs because patients will start desaturating seconds to minutes after they stop breathing.

      2. EtCO₂ monitoring provides early detection of airway compromise and can rapidly identify apnea, airway obstruction, bronchospasm, and laryngospasm. Respiratory depression can therefore be identified prior to hypoxia.

   3. Cardiopulmonary resuscitation (CPR):

      1. Monitoring of ventilation:

         1. Monitoring of the respiratory rate can be achieved more accurately with an EtCO₂ waveform. It is important not to hyperventilate patients during CPR as this leads to worse outcomes.

      2. Monitoring of effectiveness of chest compressions:

         1. In low flow states, the EtCO₂ value is a reflection of the cardiac output to the lungs. The more effective chest compressions are, the higher the EtCO₂ value will be.

      3. Assessment of return of spontaneous circulation (ROSC):

         1. A sudden increase in EtCO₂ can represent a return of spontaneous circulation and indicates the need to check for the presence of a pulse.

      4. Prognosis:

         1. EtCO₂ can be used to help determine whether further resuscitation efforts are futile as studies have shown that an EtCO₂ <10 mmHg after 20 minutes of CPR is predictive of a failure to resuscitate.

5. Monitoring conditions in which arterial PaCO₂ levels are critical:

   1. Traumatic brain injury or intracerebral hemorrhage with elevated intracranial pressure.

   2. Severely acidemic patients prior to intubation.

   3. In normal lungs with normal gas exchange, EtCO₂ values are usually 3–5 mmHg lower than arterial PaCO₂ values. In critically ill patients the values will not correlate. However, if an arterial PaCO₂ and EtCO₂ values are obtained simultaneously, EtCO₂ may be used to trend PaCO₂ values.

Ultrasonographic assessment of the inferior vena cava (IVC)

Ultrasonography of the IVC can be useful in determining fluid responsiveness. After bringing the IVC into sagittal view, changes in the diameter of the vessel with respiration are recorded. Interpretation of these measurements will depend on whether the patient is mechanically ventilated or breathing spontaneously.

1. In a spontaneously breathing patient:

   1. Assess the diameter of the IVC and percentage of collapse with inspiratory effort. This provides an estimate of central venous pressure (CVP).

   2. An IVC diameter ≤1.7 cm with complete inspiratory collapse demonstrates a low CVP (<5 mmHg).

   3. An IVC diameter of >1.7 cm with no inspiratory collapse is indicative of a high CVP (>15 mmHg).

2. In a mechanically ventilated patient:

   1. Mechanical ventilation causes the diameter of the IVC to increase with inspiration. Therefore the physician should not evaluate for IVC collapse but rather for IVC distension with inspiration.

   2. The IVC distensibility index is determined as (Maximum IVC diameter − Minimum IVC diameter)/(Minimum IVC diameter).

   3. Values ≥18% are predictive of fluid responsiveness.

3. Pitfalls:

   1. The IVC may be difficult to visualize in obese patients.

   2. Large fluctuations in intrathoracic pressure (i.e., patients in respiratory distress) will cause changes in the IVC diameter that are not a result of the patient’s volume status.